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单次高剂量和多次低剂量链脲佐菌素对糖尿病抗性和易感性大鼠心室肌细胞收缩及细胞内钙离子的影响。

Effects of single high-dose and multiple low-dose streptozotocin on contraction and intracellular Ca2+ in ventricular myocytes from diabetes resistant and susceptible rats.

作者信息

Howarth F C, Qureshi A, Shahin A, Lukic M L

机构信息

Department of Physiology, Faculty of Medicine & Health Sciences, United Arab Emirates University, Al Ain, UAE.

出版信息

Mol Cell Biochem. 2005 Jan;269(1-2):103-8. doi: 10.1007/s11010-005-3088-y.

Abstract

Administration of a single high-dose (SHD) of streptozotocin (STZ) to young adult rats causes a diabetic cardiomyopathy. Albino Oxford (AO) and Dark Agouti (DA) inbred strains of rats are susceptible to developing diabetes when administered a SHD of STZ but differ in susceptibility to multiple low-dose (MLD) STZ. We have investigated the effects of SHD and MLD-STZ on contraction and intracellular Ca2+, measured with fura-2, in ventricular myocytes from AO and DA rats at 18-20 weeks after treatment. Time to peak shortening was significantly prolonged in myocytes from DA rats after SHD-STZ but was not altered in DA rats after MLD-STZ or in AO rats by either MLD or SHZ-STZ treatment. Time to peak shortening in myocytes from DA control and DA rats after SHD-STZ were 88+/-2 ms and 107+/-4 ms, respectively. Time to half relaxation and the amplitude of myocyte shortening were not altered in AO or DA rats by either MLD or SHD-STZ treatment. Amplitude, time to peak fura-2 transient and time to half relaxation of the fura-2 transient were not significantly altered in AO or DA rats by either MLD or SHD-STZ treatment. Contractile defects reported in myocytes from SHD-STZ treated DA rats may be a consequence of altered myofilament sensitivity to Ca2+. The hyperglycaemic effects of MLD-STZ and SHD-STZ induced diabetes was much greater in DA compared to AO rats and the effects of the hyperglycaemia on the time-course of ventricular myocyte contraction was most profound in DA rats after SHD-STZ.

摘要

给年轻成年大鼠单次大剂量(SHD)注射链脲佐菌素(STZ)会导致糖尿病性心肌病。白化牛津(AO)和深色刺豚鼠(DA)近交系大鼠在接受单次大剂量STZ时易患糖尿病,但对多次低剂量(MLD)STZ的易感性不同。我们研究了单次大剂量和多次低剂量STZ对AO和DA大鼠心室肌细胞收缩及细胞内Ca2+(用fura-2测量)的影响,实验在治疗后18 - 20周进行。单次大剂量STZ处理后,DA大鼠心肌细胞的峰值缩短时间显著延长,但多次低剂量STZ处理后的DA大鼠或单次大剂量及多次低剂量STZ处理后的AO大鼠的峰值缩短时间均未改变。DA对照大鼠和单次大剂量STZ处理后的DA大鼠心肌细胞的峰值缩短时间分别为88±2毫秒和107±4毫秒。多次低剂量或单次大剂量STZ处理均未改变AO或DA大鼠心肌细胞的半松弛时间及缩短幅度。多次低剂量或单次大剂量STZ处理均未显著改变AO或DA大鼠fura-2瞬变的幅度、峰值时间及半松弛时间。单次大剂量STZ处理的DA大鼠心肌细胞中报道的收缩缺陷可能是肌丝对Ca2+敏感性改变的结果。与AO大鼠相比,多次低剂量和单次大剂量STZ诱导的糖尿病对DA大鼠的高血糖作用更强,且高血糖对心室肌细胞收缩时间进程的影响在单次大剂量STZ处理后的DA大鼠中最为显著。

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